Oncogenesis Following Delivery of a Nonprimate Lentiviral Gene Therapy Vector to Fetal and Neonatal Mice

Gene therapy by use of integrating vectors carrying therapeutic transgene sequences offers the potential for a permanent cure of genetic diseases by stable vector insertion into the patients' chromosomes. However, three cases of T cell lymphoproliferative disease have been identified almost 3 y...

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Veröffentlicht in:Molecular therapy 2005-10, Vol.12 (4), p.763-771
Hauptverfasser: Themis, Mike, Waddington, Simon N, Schmidt, Manfred, von Kalle, Christof, Wang, Yoahe, Al-Allaf, Faisal, Gregory, Lisa G, Nivsarkar, Megha, Themis, Matthew, Holder, Maxine V, Buckley, Suzanne M K, Dighe, Niraja, Ruthe, Alaine T, Mistry, Ajay, Bigger, Brian, Rahim, Ahad, Nguyen, Tuan H, Trono, Didier, Thrasher, Adrian J, Coutelle, Charles
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Sprache:eng
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Zusammenfassung:Gene therapy by use of integrating vectors carrying therapeutic transgene sequences offers the potential for a permanent cure of genetic diseases by stable vector insertion into the patients' chromosomes. However, three cases of T cell lymphoproliferative disease have been identified almost 3 years after retrovirus gene therapy for X-linked severe combined immune deficiency. In two of these cases vector insertion into the LMO2 locus was implicated in leukemogenesis, demonstrating that a more profound understanding is required of the genetic and molecular effects imposed on the host by vector integration or transgene expression. In vivo models to test for retro- and lentiviral vector safety prior to clinical application are therefore needed. Here we present a high incidence of lentiviral vector-associated tumorigenesis following in utero and neonatal gene transfer in mice. This system may provide a highly sensitive model to investigate integrating vector safety prior to clinical application.
ISSN:1525-0016
1525-0024
DOI:10.1016/j.ymthe.2005.07.358